A genome-wide association study in Han Chinese identifies multiple susceptibility loci for IgA nephropathy

Yu, Xue; Li, Ming; Zhang, Hong; Low, Hui Qi; Wei, Xin; Wang, Jin Quan; Sun, Liang; Sim, Kar Seng; Li, Yang; Foo, Jia Nee; Wang, Wei; Li, Zhi Jian; Xian, Yin; Tang, Xiaodong; Fan, Li; Chen, Jian; Li, Rong Shan; Wan, Jian; Liu, Zhang Suo; Lou, Tan Qi; Zhu, Li; Huang, Xiao Jun; Zhang, Xue Jun; Liu, Fei; Liu, Jing

doi:10.1038/ng.1047

Cited by 257 publications

(282 citation statements)

References 46 publications

Supporting

Mentioning

263

Contrasting

Unclassified

Order By: Relevance

“…We manually curated a list of SNPs that both passed genome-wide significance and were associated with kidney disease traits (Table S7). [8][9][10][11][12][13][14][15][16][17][18][19][20][21][22][23][24][25] To acquire independent loci, we removed any SNPs having r 2 R 0.2. In total, we analyzed 110 leading SNPs and 2,357 tagging SNPs with r 2 R 0.8 (Table S7).…”

Section: Kidney Eqtl Highlights the Genetics Of Disease Traitsmentioning

confidence: 99%

Genetic-Variation-Driven Gene-Expression Changes Highlight Genes with Important Functions for Kidney Disease

Qiu

et al. 2017

The American Journal of Human Genetics

View full text Add to dashboard Cite

Chronic kidney disease (CKD) is a complex gene-environmental disease affecting close to 10% of the US population. Genome-wide association studies (GWASs) have identified sequence variants, localized to non-coding genomic regions, associated with kidney function. Despite these robust observations, the mechanism by which variants lead to CKD remains a critical unanswered question. Expression quantitative trait loci (eQTL) analysis is a method to identify genetic variation associated with gene expression changes in specific tissue types. We hypothesized that an integrative analysis combining CKD GWAS and kidney eQTL results can identify candidate genes for CKD. We performed eQTL analysis by correlating genotype with RNA-seq-based gene expression levels in 96 human kidney samples. Applying stringent statistical criteria, we detected 1,886 genes whose expression differs with the sequence variants. Using direct overlap and Bayesian methods, we identified new potential target genes for CKD. With respect to one of the target genes, lysosomal beta A mannosidase (MANBA), we observed that genetic variants associated with MANBA expression in the kidney showed statistically significant colocalization with variants identified in CKD GWASs, indicating that MANBA is a potential target gene for CKD. The expression of MANBA was significantly lower in kidneys of subjects with risk alleles. Suppressing manba expression in zebrafish resulted in renal tubule defects and pericardial edema, phenotypes typically induced by kidney dysfunction. Our analysis shows that gene-expression changes driven by genetic variation in the kidney can highlight potential new target genes for CKD development.

show abstract

Section: Kidney Eqtl Highlights the Genetics Of Disease Traitsmentioning

confidence: 99%

Genetic-Variation-Driven Gene-Expression Changes Highlight Genes with Important Functions for Kidney Disease

Qiu

et al. 2017

The American Journal of Human Genetics

View full text Add to dashboard Cite

show abstract

“…Many LGWS and GWAS in both familial and sporadic IgAN suggest that there is a strong genetic component in the disease. [7][8][9][10][11][12] However, most studies have not evaluated the contribution to this complex disorder of other forms of genetic variation, such as structural variations, mainly in the form of CNVs. 15 Indeed, CNVs have recently been shown to have an important role in complex disease phenotypes as psoriasis, 30 rheumatoid arthritis 31 and systemic lupus erythematosus.…”

Section: Discussionmentioning

confidence: 99%

“…)del, containing the COL11A2 (collagen, type XI, alpha 2 isoform 1), were found in very close proximity to SNPs that gave multiple associations in the MHC class I region and HLA complex group genes identified by three independent GWAS. [10][11][12] Moreover, the loss chr6.hg18:g.(?_134 801-335)_(134 848 458_? )del overlapped with the region named IGAN1 identified in a GWLS.…”

Section: Identification Of Concordant Aberrations In Igan Patientsmentioning

confidence: 99%

“…Three GWLS of familial IgAN have reported linkages at 2q36, 4q26-31, 6q22-23 and 17q12-22, but no disease genes were identified within these areas. [7][8][9] Three GWAS that allows hypothesis-free examination have been performed for IgAN, leading to the identification of susceptibility alleles in the major histocompatibility complex (MHC) region on chromosome 6p [10][11][12] and additional loci on chromosomes 1q32, 22q12, 17p13 and 8p23. So far, no genetic variants or genes underlying these loci have been identified as causative or affecting the pathology, plausibly because of the presence of genetic/environmental and locus heterogeneity and to contribution from noncoding susceptibility alleles such as point mutations or structural genomic variants within intronic or promoter regions.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Genome-wide scan identifies a copy number variable region at 3p21.1 that influences the TLR9 expression levels in IgA nephropathy patients

et al. 2014

View full text Add to dashboard Cite

on behalf of the European IgAN ConsortiumImmunoglobulin A nephropathy (IgAN) is a complex multifactorial disease characterized by genetic factors that influence the pathogenesis of the disease. In this context, an intriguing role could be ascribed to copy number variants (CNVs). We performed the whole-genome screening of CNVs in familial IgAN patients, their healthy relatives and healthy subjects (HSs). In the initial screening, we included 217 individuals consisting of 51 biopsy-proven familial IgAN cases and 166 healthy relatives. We identified 148 IgAN-specific aberrations, specifically 105 loss and 43 gain, using a new statistical approach that allowed us to identify aberrations that were concordant across multiple samples. Several CNVs overlapped with regions evidenced by previous genome-wide genetic studies. We focused our attention on a CNV located in chromosome 3, which contains the TLR9 gene and found that IgAN patients characterized by deteriorated renal function carried low copy number of this CNV. Moreover, the TLR9 gene expression was low and significantly correlated with the loss aberration. Conversely, IgAN patients with normal renal function had no aberration and the TLR9 mRNA was expressed at the same level as in HSs. We confirmed our data in another cohort of Greek subjects. In conclusion, here we performed the first genome-wide CNV study in IgAN identifying structural variants that could help the genetic dissection of this complex disease, and pointed out a loss aberration in the chromosome 3, which is responsible for the downregulation of TLR9 expression that, in turn, could contribute to the deterioration of the renal function in IgAN patients.

show abstract

“…Association studies identified distinct loci on chromosomes 6p21, 8p23, 17p13, 22q12, 1q32. 6,7 On the other hand, classical linkage studies performed on AD families identified additional loci on chromosomes 2q36, 4q26-31, 6q22, 17q12-22, [8][9][10] lending further support to the complex etiology and broad genetic heterogeneity of the disease.…”

Section: Introductionmentioning

confidence: 88%

A SPRY2 mutation leading to MAPK/ERK pathway inhibition is associated with an autosomal dominant form of IgA nephropathy

Milillo¹,

Carpia²,

Costanzi

et al. 2015

Eur J Hum Genet

View full text Add to dashboard Cite

IgA nephropathy (IgAN) represents the most common primary glomerulonephritis worldwide with a prevalence of 25-50% among patients with primary glomerulopathies. In~5-10% of the patients the disease segregates with an autosomal dominant (AD) pattern. Association studies identified loci on chromosomes 1q32, 6p21, 8p23, 17p13, 22q12, whereas classical linkage studies on AD families identified loci on chromosomes 2q36, 4q26-31, 6q22, 17q12-22. We have studied a large Sicilian family where IgAN segregates with an AD transmission. To identify the causal gene, the exomes of two affected and one unaffected individual have been sequenced. From the bioinformatics analysis a p.(Arg119Trp) variant in the SPRY2 gene was identified as the probable disease-causing mutation. Moreover, functional characterization of this variant showed that it is responsible for the inhibition of the MAPK/ERK1/2 pathway. The same effect was observed in two sporadic IgAN patients carriers of wild-type SPRY2, suggesting that downregulation of the MAPK/ERK1/2 pathway represents a common mechanism leading to IgAN.

show abstract

A genome-wide association study in Han Chinese identifies multiple susceptibility loci for IgA nephropathy

Cited by 257 publications

References 46 publications

Genetic-Variation-Driven Gene-Expression Changes Highlight Genes with Important Functions for Kidney Disease

Genetic-Variation-Driven Gene-Expression Changes Highlight Genes with Important Functions for Kidney Disease

Genome-wide scan identifies a copy number variable region at 3p21.1 that influences the TLR9 expression levels in IgA nephropathy patients

A SPRY2 mutation leading to MAPK/ERK pathway inhibition is associated with an autosomal dominant form of IgA nephropathy

Contact Info

Product

Resources

About